The human gut microbiota contributes to type-2 diabetes non-resolution 5-years after Roux-en-Y gastric bypass

2型糖尿病 肠道菌群 Roux-en-Y吻合术 脆弱类杆菌 生物 内科学 拟杆菌 队列 肥胖 减肥 胃分流术 失调 胃肠病学 糖尿病 粪便 生理学 内分泌学 医学 免疫学 细菌 微生物学 遗传学
作者
Jean Debédat,Tiphaine Le Roy,Lise Voland,Eugeni Belda,Rohia Alili,Solia Adriouch,Pierre Bel Lassen,Kazuyuki Kasahara,Evan Hutchison,Laurent Genser,Lícia Torres,Camille Gamblin,Christine Rouault,Jean-Daniel Zucker,Nathalie Kapel,Christine Poitou,Geneviève Marcelin,Federico E. Rey,Judith Aron‐Wisnewsky,Karine Clément
出处
期刊:Gut microbes [Landes Bioscience]
卷期号:14 (1) 被引量:11
标识
DOI:10.1080/19490976.2022.2050635
摘要

Roux-en-Y gastric bypass (RYGB) is efficient at inducing drastic albeit variable weight loss and type-2 diabetes (T2D) improvements in patients with severe obesity and T2D. We hypothesized a causal implication of the gut microbiota (GM) in these metabolic benefits, as RYGB is known to deeply impact its composition. In a cohort of 100 patients with baseline T2D who underwent RYGB and were followed for 5-years, we used a hierarchical clustering approach to stratify subjects based on the severity of their T2D (Severe vs Mild) throughout the follow-up. We identified via nanopore-based GM sequencing that the more severe cases of unresolved T2D were associated with a major increase of the class Bacteroidia, including 12 species comprising Phocaeicola dorei, Bacteroides fragilis, and Bacteroides caecimuris. A key observation is that patients who underwent major metabolic improvements do not harbor this enrichment in Bacteroidia, as those who presented mild cases of T2D at all times. In a separate group of 36 patients with similar baseline clinical characteristics and preoperative GM sequencing, we showed that this increase in Bacteroidia was already present at baseline in the most severe cases of T2D. To explore the causal relationship linking this enrichment in Bacteroidia and metabolic alterations, we selected 13 patients across T2D severity clusters at 5-years and performed fecal matter transplants in mice. Our results show that 14 weeks after the transplantations, mice colonized with the GM of Severe donors have impaired glucose tolerance and insulin sensitivity as compared to Mild-recipients, all in the absence of any difference in body weight and composition. GM sequencing of the recipient animals revealed that the hallmark T2D-severity associated bacterial features were transferred and were associated with the animals’ metabolic alterations. Therefore, our results further establish the GM as a key contributor to long-term glucose metabolism improvements (or lack thereof) after RYGB.

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